Trending

Scientists have long questioned whether the abundant amounts ofamyloid plaques found in the brains of patients with Alzheimer’s
actually caused the neurological disease or were a by-product of its
progress. Now, using new research techniques, scientists have shown
that a two-molecule aggregate (or dimer) of beta-amyloid protein
fragments may play a role in initiating the disease.

Alzheimer’s disease is marked by the build-up of plaques
consisting of beta-amyloid protein fragments, as well as abnormal
tangles of tau protein found inside brain cells. Early in the
disease, Alzheimer’s pathology is first observed in the hippocampus,
the part of the brain important to memory, and gradually spreads to
the cerebral cortex, the outer layer of the brain.

In this study, in which the Harvard and Brigham team collaborated with other Harvard researchers and scientists at University College Dublin, Beaumont Hospital and Royal College of
Surgeons Ireland, and Trinity College Dublin, Ireland,
researchers tested cerebral cortex extracts from brains donated for
autopsy by people aged 65 and older with Alzheimer’s and other
dementias, as well as those without dementia. The extracts contained
soluble one-molecule (monomer), two-molecule (dimer), three-molecule
(trimer) or larger aggregates of beta-amyloid, as well as insoluble
plaque cores. The researchers then injected the extracts into normal
rats or added the extracts to slices of normal mouse hippocampus.

Selkoe, lead author Ganesh M. Shankar and colleagues discovered that both the soluble
monomers and the insoluble plaque cores had no detectable effect on
the hyppocampal slices. However, the soluble dimers induced certain
key characteristics of Alzheimer’s in the rats. The dimers impaired
memory function, specifically the memories of newly learned
behaviors.

In the mouse hippocampal slices, the dimers also reduced
by 47 percent the density of the dendrite spines that receive
messages sent by other brain cells. The dimers seemed to be directly
acting on synapses, the connections between neurons that are
essential for communication between them.

To confirm this effect, the researchers then injected certain
antibodies against beta-amyloid protein fragments. These latched
onto and inactivated the dimers, preventing their toxic effects in
the animal models. However, much work remains to be done before
inactivation of dimers could move into the clinic.

“Scientists have theorized for many years that soluble
beta-amyloid may be critical to the development and progression of
this devastating disease. Now these researchers have isolated a
candidate causative agent from brains of people with typical
Alzheimer’s and directly tested it in an animal model,” said Richard J. Hodes, M.D., Director of the National Institute on Aging(NIA), which financed the research. “While more research is needed to
replicate and extend these findings,” Hodes said, “this study has put yet one more
piece into place in the puzzle that is Alzheimer’s.”

The animal findings were consistent with what the researchers
found when they examined the brain tissues of people who had been
clinically diagnosed with Alzheimer’s and those without dementia.
They detected soluble dimers and some trimers of amyloid in the
brains of patients with Alzheimer’s, but none or very low levels in
those free of the disorder. Some people free of the disorder,
however, did have insoluble amyloid plaques in their brains.

“These findings may help explain why people with normal cognitive
function are sometimes found to have large amounts of amyloid
plaques in their brains, which has been a puzzle for some time,”
said Marcelle Morrison-Bogorad, director of the NIA Division
of Neuroscience. “Their findings noted that the brain of an
individual who was never clinically diagnosed with dementia was
found with abundant insoluble Alzheimer’s plaques, but no soluble
beta-amyloid.”

Selkoe and Shankar noted that further insights into the early
stages of this disease process may answer questions not only about
Alzheimer’s, but also about age-related memory impairments. “The
approaches we used to isolate dimers and the widespread availability
of tissues from brain banks, open new avenues of investigation into
how these aggregates induce Alzheimer’s disease,” said Selkoe. “We
still need to find out why dimers in particular are so destructive
to neurons.”